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Two dual specificity kinases are preferentially induced by wild-type rather than by oncogenic RAS-P21 in Xenopus oocytes

  • Yongxia Qu
  • , Victor Adler
  • , Tearina Chu
  • , Ovidu Platica
  • , Josef Michl
  • , Sidney Pestka
  • , Lara Izotova
  • , Mohamed Boutjdir
  • , Matthew R. Pincus

Research output: Contribution to journalArticlepeer-review

7 Scopus citations

Abstract

In prior studies, we have found that oncogenic ras-p21 protein induces oocyte maturation using pathways that differ from those activated by insulin-induced wild-type ras-p21. Both oncogenic and wild-type ras-p21 require interactions with raf, but unlike oncogenic ras-p21, insulin-activated wild-type ras-p21 does not depend completely on activation of MEK and MAP kinase (MAPK or ERK) on the raf kinase pathway. To determine what raf-dependent but MAPK-independent pathway is activated by wild-type ras-p21, we have analyzed gene expression in oocytes induced to mature either with oncogenic ras-p21 or with insulin using a newly available Xenopus gene array. We find a number of proteins that are preferentially expressed in one or the other system. Of these, two proteins, both dual function kinases, T-Cell Origin Protein Kinase (TOPK) and the nuclear kinase, DYRK1A, are preferentially expressed in the insulin system. Confirming this finding, blots of lysates of oocytes, induced to mature with oncogenic ras-p21 and insulin, with anti-TOPK and anti-DYRK1A show much higher protein expression in the lysates from the insulin-matured oocytes. Neither of these kinases activates or is activated by MAPK and is therefore an attractive candidate for being on a signal transduction pathway that is unique to insulin-activated wildtype ras-p21-induced oocyte maturation.

Original languageEnglish
Pages (from-to)2420-2427
Number of pages8
JournalFrontiers in bioscience : a journal and virtual library
Volume11
Issue numberSUPPL. 2
DOIs
StatePublished - 2006

Keywords

  • Dual Specificity Kinase
  • Gene Expression
  • Gene array
  • Insulin-Activated Wild-Type Ras-P21
  • Oncogene
  • Oncogenic Ras-P21
  • Oocyte Maturation
  • Protein Expression
  • Signal Transduction Pathways
  • Xenopus

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